Disruption of the Tumour-associated EMP3 Enhances Erythroid Proliferation and Causes the MAM-negative Phenotype

Overview

Journal Nat Commun

Specialty Biology

Date 2020 Jul 18

PMID 32678083

Citations 14

Authors

Nicole Thornton

Vanja Karamatic Crew

Louise Tilley

Carole A Green

Chwen Ling Tay

Rebecca E Griffiths

Belinda K Singleton

Frances Spring

Piers Walser

Abdul Ghani Alattar

Benjamin Jones

Rosalind Laundy

Jill R Storry

Mattias Moller

Lorna Wall

Richard Charlewood

Connie M Westhoff

Christine Lomas-Francis

Vered Yahalom

Ute Feick

Axel Seltsam

Beate Mayer

Martin L Olsson

David J Anstee

Affiliations

Soon will be listed here.

Abstract

The clinically important MAM blood group antigen is present on haematopoietic cells of all humans except rare MAM-negative individuals. Its molecular basis is unknown. By whole-exome sequencing we identify EMP3, encoding epithelial membrane protein 3 (EMP3), as a candidate gene, then demonstrate inactivating mutations in ten known MAM-negative individuals. We show that EMP3, a purported tumour suppressor in various solid tumours, is expressed in erythroid cells. Disruption of EMP3 by CRISPR/Cas9 gene editing in an immortalised human erythroid cell line (BEL-A2) abolishes MAM expression. We find EMP3 to associate with, and stabilise, CD44 in the plasma membrane. Furthermore, cultured erythroid progenitor cells from MAM-negative individuals show markedly increased proliferation and higher reticulocyte yields, suggesting an important regulatory role for EMP3 in erythropoiesis and control of cell production. Our data establish MAM as a new blood group system and demonstrate an interaction of EMP3 with the cell surface signalling molecule CD44.

Citing Articles

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